Use of Reverse Phase Protein Microarrays and Reference Standard Development for Molecular Network Analysis of Metastatic Ovarian Carcinoma

Katherine M. Sheehan(National Institutes of Health), Valerie Calvert(Center for Biologics Evaluation and Research), Elaine W. Kay(Royal College of Surgeons in Ireland), Yiling Lu(The University of Texas MD Anderson Cancer Center), David A. Fishman(New York University), Virginia Espina(National Institutes of Health), Joy Aquino(Center for Biologics Evaluation and Research), Runa Speer(National Institutes of Health), Robyn P. Araujo(National Institutes of Health), Gordon B. Mills(The University of Texas MD Anderson Cancer Center), Lance A. Liotta(National Institutes of Health), Emanuel F. Petricoin(Center for Biologics Evaluation and Research), Julia Wulfkuhle(National Institutes of Health)
Molecular & Cellular Proteomics
January 30, 2005
Cited by 310Open Access
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Abstract

Cancer can be defined as a deregulation or hyperactivity in the ongoing network of intracellular and extracellular signaling events. Reverse phase protein microarray technology may offer a new opportunity to measure and profile these signaling pathways, providing data on post-translational phosphorylation events not obtainable by gene microarray analysis. Treatment of ovarian epithelial carcinoma almost always takes place in a metastatic setting since unfortunately the disease is often not detected until later stages. Thus, in addition to elucidation of the molecular network within a tumor specimen, critical questions are to what extent do signaling changes occur upon metastasis and are there common pathway elements that arise in the metastatic microenvironment. For individualized combinatorial therapy, ideal therapeutic selection based on proteomic mapping of phosphorylation end points may require evaluation of the patient's metastatic tissue. Extending these findings to the bedside will require the development of optimized protocols and reference standards. We have developed a reference standard based on a mixture of phosphorylated peptides to begin to address this challenge.


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